Ferroxitosis: A cell death from modulation of oxidative phosphorylation and PKM2-dependent glycolysis in melanoma

Reliance on glycolysis is a characteristic of malignancy, yet the development of resistance to BRAF inhibitors in melanoma is associated with gain of mitochondrial function. Concurrent attenuation of oxidative phosphorylation and HIF-1α/PKM2-dependent glycolysis promotes a non-apoptotic, iron- and o...

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Autores principales: Lakhter, Alexander J., Hamilton, James, Dagher, Pierre C., Mukkamala, Suresh, Hato, Takashi, Dong, X. Charlie, Mayo, Lindsey D., Harris, Robert A., Shekhar, Anantha, Ivan, Mircea, Brustovetsky, Nickolay, Naidu, Samisubbu R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2014
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4350353/
https://www.ncbi.nlm.nih.gov/pubmed/25587028
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author Lakhter, Alexander J.
Hamilton, James
Dagher, Pierre C.
Mukkamala, Suresh
Hato, Takashi
Dong, X. Charlie
Mayo, Lindsey D.
Harris, Robert A.
Shekhar, Anantha
Ivan, Mircea
Brustovetsky, Nickolay
Naidu, Samisubbu R.
author_facet Lakhter, Alexander J.
Hamilton, James
Dagher, Pierre C.
Mukkamala, Suresh
Hato, Takashi
Dong, X. Charlie
Mayo, Lindsey D.
Harris, Robert A.
Shekhar, Anantha
Ivan, Mircea
Brustovetsky, Nickolay
Naidu, Samisubbu R.
author_sort Lakhter, Alexander J.
collection PubMed
description Reliance on glycolysis is a characteristic of malignancy, yet the development of resistance to BRAF inhibitors in melanoma is associated with gain of mitochondrial function. Concurrent attenuation of oxidative phosphorylation and HIF-1α/PKM2-dependent glycolysis promotes a non-apoptotic, iron- and oxygen-dependent cell death that we term ferroxitosis. The redox cycling agent menadione causes a robust increase in oxygen consumption, accompanied by significant loss of intracellular ATP and rapid cell death. Conversely, either hypoxic adaptation or iron chelation prevents menadione-induced ferroxitosis. Ectopic expression of K213Q HIF-1α mutant blunts the effects of menadione. However, knockdown of HIF-1α or PKM2 restores menadione-induced cytotoxicity in hypoxia. Similarly, exposure of melanoma cells to shikonin, a menadione analog and a potential PKM2 inhibitor, is sufficient to induce ferroxitosis under hypoxic conditions. Collectively, our findings reveal that ferroxitosis curtails metabolic plasticity in melanoma.
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spelling pubmed-43503532015-03-06 Ferroxitosis: A cell death from modulation of oxidative phosphorylation and PKM2-dependent glycolysis in melanoma Lakhter, Alexander J. Hamilton, James Dagher, Pierre C. Mukkamala, Suresh Hato, Takashi Dong, X. Charlie Mayo, Lindsey D. Harris, Robert A. Shekhar, Anantha Ivan, Mircea Brustovetsky, Nickolay Naidu, Samisubbu R. Oncotarget Research Paper Reliance on glycolysis is a characteristic of malignancy, yet the development of resistance to BRAF inhibitors in melanoma is associated with gain of mitochondrial function. Concurrent attenuation of oxidative phosphorylation and HIF-1α/PKM2-dependent glycolysis promotes a non-apoptotic, iron- and oxygen-dependent cell death that we term ferroxitosis. The redox cycling agent menadione causes a robust increase in oxygen consumption, accompanied by significant loss of intracellular ATP and rapid cell death. Conversely, either hypoxic adaptation or iron chelation prevents menadione-induced ferroxitosis. Ectopic expression of K213Q HIF-1α mutant blunts the effects of menadione. However, knockdown of HIF-1α or PKM2 restores menadione-induced cytotoxicity in hypoxia. Similarly, exposure of melanoma cells to shikonin, a menadione analog and a potential PKM2 inhibitor, is sufficient to induce ferroxitosis under hypoxic conditions. Collectively, our findings reveal that ferroxitosis curtails metabolic plasticity in melanoma. Impact Journals LLC 2014-12-26 /pmc/articles/PMC4350353/ /pubmed/25587028 Text en Copyright: © 2014 Lakhter et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Lakhter, Alexander J.
Hamilton, James
Dagher, Pierre C.
Mukkamala, Suresh
Hato, Takashi
Dong, X. Charlie
Mayo, Lindsey D.
Harris, Robert A.
Shekhar, Anantha
Ivan, Mircea
Brustovetsky, Nickolay
Naidu, Samisubbu R.
Ferroxitosis: A cell death from modulation of oxidative phosphorylation and PKM2-dependent glycolysis in melanoma
title Ferroxitosis: A cell death from modulation of oxidative phosphorylation and PKM2-dependent glycolysis in melanoma
title_full Ferroxitosis: A cell death from modulation of oxidative phosphorylation and PKM2-dependent glycolysis in melanoma
title_fullStr Ferroxitosis: A cell death from modulation of oxidative phosphorylation and PKM2-dependent glycolysis in melanoma
title_full_unstemmed Ferroxitosis: A cell death from modulation of oxidative phosphorylation and PKM2-dependent glycolysis in melanoma
title_short Ferroxitosis: A cell death from modulation of oxidative phosphorylation and PKM2-dependent glycolysis in melanoma
title_sort ferroxitosis: a cell death from modulation of oxidative phosphorylation and pkm2-dependent glycolysis in melanoma
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4350353/
https://www.ncbi.nlm.nih.gov/pubmed/25587028
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